Brain vasopressin and sodium appetite

Flynn, Francis W.; Kirchner, Thomas; Clinton, Margaret E

doi:10.1152/ajpregu.00181.2001

Cited by 21 publications

(20 citation statements)

References 46 publications

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“…Mineralocorticoids have further been shown to upregulate Fos (41,42), angiotensin receptors (51), oxytocin receptors (51), vasopressin (20), and the vasopressin V 1a receptor (41,42). Vasopressin (11) and angiotensin II (9,29,45,50,51) in turn stimulate, whereas oxytocin (53) inhibits, salt intake. Interestingly, the effect of mineralocorticoids or salt depletion on salt appetite may be modified by glucocorticoids (18,34,50) and amphetamine (5).…”

Section: Discussionmentioning

confidence: 99%

SGK1 as a determinant of kidney function and salt intake in response to mineralocorticoid excess

Vallon¹,

Huang²,

Grahammer³

et al. 2005

American Journal of Physiology-Regulatory, Integrative and Comp

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Section: Discussionmentioning

confidence: 99%

SGK1 as a determinant of kidney function and salt intake in response to mineralocorticoid excess

Vallon¹,

Huang²,

Grahammer³

et al. 2005

American Journal of Physiology-Regulatory, Integrative and Comp

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“…Sodium depletion was induced by injections of furosemide (7.5 mg/kg, administered subcutaneously [sc]) and deoxycorticosterone acetate (DOCA, 5 mg/kg, sc) (Flynn et al 2005), followed 2 h later by an additional injection of 7.5 mg/kg furosemide (Tamura and Norgren 1997). Pilot studies indicated that this combination induced a more robust behavioral salt appetite than either single hormone alone in our lab and therefore the combination was selected for this electrophysiological and taste reactivity study (personal observations).…”

Section: Oral Infusion Testingmentioning

confidence: 99%

Ventral Pallidum Firing Codes Hedonic Reward: When a Bad Taste Turns Good

Tindell

Smith

Peciña

et al. 2006

Journal of Neurophysiology

219

192

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The ventral pallidum (VP) is a key structure in brain mesocorticolimbic reward circuits that mediate "liking" reactions to sensory pleasures. Do firing patterns in VP actually code sensory pleasure? Strong evidence for hedonic coding requires showing that neural signals track positive increases in sensory pleasure or even reversals from bad to good. A useful test is the salt alliesthesia of physiological sodium depletion that makes even aversively intense NaCl taste become palatable and "liked." We compared VP neural firing activity in rats during aversive "disliking" reactions elicited by a noxiously intense NaCl taste (triple-seawater 1.5 M concentration) in normal homeostatic state versus in a physiological salt appetite state that made the same NaCl taste palatable and elicit positive "liking" reactions. We also compared firing elicited by palatable sucrose taste, which always elicited "liking" reactions in both states. A dramatic doubling in the amplitude of VP neural firing peaks to NaCl was caused by salt appetite that matched the affective switch from aversive ("disliking") to positive hedonic ("liking") reactions. By contrast, VP neural activity to "liked" sucrose taste was always high and never altered. In summary, VP firing activity selectively tracks the hedonic values of tastes, even across hedonic reversals caused by physiological changes. Our data provide the strongest evidence yet for neural hedonic coding of natural sensory pleasures and suggest, by extension, how abnormalities in VP firing patterns might contribute to clinical hedonic dysfunctions.

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“…Rats were removed from the home cage, administered an intraventricular injection of angiotensin II (50 g/3 l; Sigma, St. Louis, MO), and returned to the cage. Water intake was measured for 20 min, and rats were determined to have correct placement of a patent cannula if they drank Ͼ5.0 ml of water following the angiotensin II injection (13,14). The experiments began 1-2 wk later.…”

Section: Surgerymentioning

confidence: 99%

“…In addition, the neurohypophyseal hormones, oxytocin and VP, are associated with the control of sodium balance (14). More specifically, many treatments that arouse the ingestion of sodium solutions also stimulate the release of VP into the blood (15,18,22,47,55).…”

mentioning

confidence: 99%

Centrally administered vasopressin cross-sensitizes rats to amphetamine and drinking hypertonic NaCl

McBride¹,

Flynn²

2007

American Journal of Physiology-Regulatory, Integrative and Comp

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Prior sodium restriction cross-sensitizes rats to the psychomotor effects of amphetamines and vice versa. Repeated central injections of vasopressin (VP) induce a psychomotor sensitization similar to amphetamine sensitization and repeated sodium deficiency. Thus brain VP signaling may be a common mechanism involved in mediating these two motivational systems. In experiment 1, we tested the hypothesis that rats previously sensitized to central VP would show enhanced psychomotor responses to amphetamine. Rats were administered saline, VP (50 ng), or amphetamine (1 mg/kg or 3 mg/kg) on days 1 and 2, and given saline or amphetamine on day 3. Amphetamine produced psychomotor arousal in all groups. However, amphetamine on day 3 elicited a significantly greater psychomotor response in rats that had prior injections of amphetamine or VP than in rats previously treated with saline. In experiment 2, the hypothesis that prior experience with central VP would cross-sensitize rats to drinking hypertonic sodium (NaCl) solutions was tested. Rats were administered VP (50 ng) or saline for 3 days. On the fourth day, nondeprived rats were given access to 0.3 M NaCl and water for 1 h. Control and saline-treated rats only drank 1 ml of 0.3 M NaCl, but rats previously exposed to central VP drank significantly more hypertonic saline (4 ml). These results show that prior experience with central VP cross-sensitizes rats to the psychomotor stimulant effects of amphetamine and the ingestion of concentrated NaCl solutions. This pattern of cross-sensitization links central VP signaling, amphetamine, and sodium deficiency, and therefore it may play a role in the cross-sensitization between sodium appetite and amphetamines.

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Brain vasopressin and sodium appetite

Cited by 21 publications

References 46 publications

SGK1 as a determinant of kidney function and salt intake in response to mineralocorticoid excess

SGK1 as a determinant of kidney function and salt intake in response to mineralocorticoid excess

Ventral Pallidum Firing Codes Hedonic Reward: When a Bad Taste Turns Good

Centrally administered vasopressin cross-sensitizes rats to amphetamine and drinking hypertonic NaCl

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